Genotype–phenotype studies in nail-patella syndrome show that LMX1B mutation location is involved in the risk of developing nephropathy

Abstract: Nail-patella syndrome (NPS) is characterized by developmental defects of dorsal limb structures, nephropathy, and glaucoma and is caused by heterozygous mutations in the LIM homeodomain transcription factor LMX1B. In order to identify possible genotype-phenotype correlations, we performed LMX1B mutation analysis and comprehensive investigations of limb, renal, ocular, and audiological characteristics in 106 subjects from 32 NPS families. Remarkable phenotypic variability at the individual, intrafamilial, and i… Show more

“…2 There is, however, a link between genotype and phenotype; individuals with a mutation in the LMX1B homeodomain have a higher frequency of proteinuria than those with mutations in the LIM domains. 3 …”

Familial Nephropathy and Multiple Exostoses With Exostosin-1 (EXT1) Gene Mutation

“…2 There is, however, a link between genotype and phenotype; individuals with a mutation in the LMX1B homeodomain have a higher frequency of proteinuria than those with mutations in the LIM domains. 3 …”

Familial Nephropathy and Multiple Exostoses With Exostosin-1 (EXT1) Gene Mutation

“…Bu tarz patellar bozukluklar sık görülmesine rağmen, tırnak-patella sendromunda belirgin fonksiyonel yetmezlik nadiren tespit edilir. [18,19] Ek olarak, lateral femoral kondil hipoplazisi, interkondiler çentikte genişleme, lateral femoral kondilde osteokondral defekt, tibial tüberkülde belirginleşme, fibula başı hipoplazisi, genu valgum veya varum, pes ekinovarus, kalça displazisi ve büyük eklem kontraktürleri görülebilir. [17,20] Nadiren, aşırı genu valgum gelişen olgularda, düzeltici tibial osteotomilere gereksinim duyulabilir.…”

Congenital patellofemoral joint problems

“…During ischemia, reactive oxygen species (ROS) cause peroxidation of CL, and this process is enhanced by peroxidase activity of cytochrome c (a cationic component of the OXPHOS chain that is normally closely associated with anionic CL) in the presence of H 2 O 2 6 ; this causes an alteration in the structure of cristae, leading to a defect in the functional capacity of mitochondria to produce ATP. Dissociation of cytochrome c from CL can lead to its release into the cell, activation of programmed cell death pathways, and irreversible opening of the mitochondrial permeability transition pore (which, intriguingly, may be formed of dimers of ATP synthase, according to very recent research 7 ).…”

“…Other musculoskeletal abnormalities can affect muscles, tendons, and ligaments. Additional manifestations, more recently recognized, include normal pressure glaucoma and sensorineural hearing loss (7). There is considerable inter-and intrafamily variability with regard to the range of tissue manifestations (8).…”

An Expanding Universe of FSGS Genes and Phenotypes